Single-Cell CRISPR Immune Screens Reveal Immunological Roles of Tumor Intrinsic Factors

Authors

Jiakai Hou
Shaoheng Liang
Chunyu Xu
Yanjun Wei
Yunfei Wang
Yukun Tan
Nidhi Sahni
Daniel J McGrail
Chantale Bernatchez
Michael Davies
Yumei Li
Rui Chen
S Stephen Yi
Yiwen Chen
Cassian Yee
Ken Chen
Weiyi Peng

Publication Date

12-1-2022

Journal

NAR Cancer

Abstract

Genetic screens are widely exploited to develop novel therapeutic approaches for cancer treatment. With recent advances in single-cell technology, single-cell CRISPR screen (scCRISPR) platforms provide opportunities for target validation and mechanistic studies in a high-throughput manner. Here, we aim to establish scCRISPR platforms which are suitable for immune-related screens involving multiple cell types. We integrated two scCRISPR platforms, namely Perturb-seq and CROP-seq, with both in vitro and in vivo immune screens. By leveraging previously generated resources, we optimized experimental conditions and data analysis pipelines to achieve better consistency between results from high-throughput and individual validations. Furthermore, we evaluated the performance of scCRISPR immune screens in determining underlying mechanisms of tumor intrinsic immune regulation. Our results showed that scCRISPR platforms can simultaneously characterize gene expression profiles and perturbation effects present in individual cells in different immune screen conditions. Results from scCRISPR immune screens also predict transcriptional phenotype associated with clinical responses to cancer immunotherapy. More importantly, scCRISPR screen platforms reveal the interactive relationship between targeting tumor intrinsic factors and T cell-mediated antitumor immune response which cannot be easily assessed by bulk RNA-seq. Collectively, scCRISPR immune screens provide scalable and reliable platforms to elucidate molecular determinants of tumor immune resistance.

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Associated Data

PMID: 36518525